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BIOE 301

BIOE 301. Lecture One. Course Organization. People Syllabus Website: http://www.owlnet.rice.edu/~bioe301/kortum/class/ BIOE 301 Roadmap. Science of Understanding Disease. Emerging Health Technologies. Bioengineering. Preclinical Testing. Ethics of research. Adoption & Diffusion.

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BIOE 301

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  1. BIOE 301 Lecture One

  2. Course Organization • People • Syllabus • Website: • http://www.owlnet.rice.edu/~bioe301/kortum/class/ • BIOE 301 Roadmap

  3. Science of Understanding Disease Emerging Health Technologies Bioengineering Preclinical Testing Ethics of research Adoption & Diffusion Clinical Trials • Abandoned due to: • poor performance • safety concerns • ethical concerns • legal issues • social issues • economic issues Cost-Effectiveness

  4. Four Questions • What are the problems in healthcare today? • Who pays to solve problems in healthcare? • How can we use science and technology to solve healthcare problems? • Once developed, how do new healthcare technologies move from the lab to the bedside? • BIOE 301 Concept map

  5. Mortality Ages 0-4: Perinatal conditions Lower respiratory infections Diarrheal diseases Malaria Perinatal conditions Congenital anomalies Lower respiratory infections Unintentional injuries Ages 15-44: HIV/AIDS Unintentional injuries Cardiovascular diseases Tuberculosis Unintentional injuries Cardiovascular disease Cancer Self-Inflicted Injuries   Ages 45-59: Cardiovascular diseases Cancers Unintentional injuries HIV/AIDS Cardiovascular diseases Cancer Unintentional injuries Digestive Diseases

  6. Ovary

  7. Technology Assessment • What is it? • Why do we need it? • Example • Bone marrow transplants for breast cancer

  8. Your Situation • You have just been diagnosed with advanced cancer • Your physician tells you that with standard treatment, there is only a 15% chance that you will survive 5 years. • She informs you that she is testing a new therapy which may increase your chance of surviving 5 years by more than 40%. • The new therapy has extremely painful side effects and there is limited scientific evidence that it works. • The new therapy costs $150,000 and your insurance company refuses to pay for it. • What do you do?

  9. Technology Assessment: Overview • The disease: • Breast Cancer • The technology: • High dose chemotherapy (HDCT) with autologous stem cell support (ASCS) • $80,000-$150,000, high morbidity, initially high mortality • The assessment: • 1980s: Small clinical trials promising • Many patients demanded treatment even though there was very little evidence that it worked • What happened next?

  10. The Disease • Breast Cancer • 211,240 new cases of breast cancer will be diagnosed in the U.S. in 2005 • Over 2.3 million women living in the U.S. who have been diagnosed with & treated for breast cancer • 2nd leading cause of cancer death among women in the U.S. • Incidence and mortality rates vs. time

  11. http://cwx.prenhall.com/bookbind/pubbooks/silverthorn2/medialib/Image_Bank/CH24/FG24_22a.jpg http://cwx.prenhall.com/bookbind/pubbooks/silverthorn2/medialib/Image_Bank/CH22/FG22_02a.jpg

  12. Breast Cancer Staging

  13. Treatments for Breast Cancer • Surgery • Lumpectomy • Mastectomy • Used to remove small tumors • Chemotherapy • May be used to shrink larger tumors so that they can be removed surgically • May be used following surgery to reduce risk of recurrence • May be used to treat stage IV breast cancer • e.g. cyclophosphamide with doxorubicin or epirubicin • Radiation Therapy • May be used following surgery to reduce risk of recurrence • Hormone Therapy • May be used to shrink larger estrogen positive tumors so that they can be removed surgically • May be used following surgery to reduce risk of recurrence • e.g. Tamoxifen – an anti-estrogen drug

  14. The Technology • High dose chemotherapy (HDCT) with autologous stem cell support (ASCS) • How does chemo work? • How does high dose chemo work? • Why do we need ASCS? • Bone marrow transplants • What are they? • How were they developed?

  15. Chemotherapy • How does it work? • Chemotherapy drugs given IV or by mouth • They travel through the bloodstream to reach cancer cells in most parts of the body • Interfere with ability of cell to divide • Cancer cells cannot repair damage caused by chemotherapy drugs so they die • Rapidly dividing normal cells may also be affected by chemo drugs but they can repair this damage • Possible Side effects • Temporary: Nausea and vomiting, loss of appetite, hair loss, mouth sores, low blood cell count (infection, bleeding, fatigue) • Permanent: Premature menopause and infertility

  16. High Dose Chemotherapy • Dose of chemotherapy • Balance between goal of completely destroying all cancer cells & causing too much damage to normal cells • Dose comparison studies of chemo in metastatic breast cancer show high dose is associated with high response rate • High dose chemotherapy (HDCT) • Wipe out cancer cells with extremely high doses of chemotherapy • Such doses also destroy bone marrow, including stem cells that eventually mature into cells of the blood and immune system • Patients receiving HDCT must undergo a transplant to restore the bone marrow cells

  17. Bone Marrow Transplants • Components of blood • Plasma • Cells • Red blood cells • White blood cells • Platelets • Cells are produced in the bone marrow from pluripotent hematopoeitic stem cells • Lab expts: a single stem cell can yield the half-trillion blood cells of an entire mouse

  18. http://cwx.prenhall.com/bookbind/pubbooks/silverthorn2/medialib/Image_Bank/CH16/FG16_03.jpghttp://cwx.prenhall.com/bookbind/pubbooks/silverthorn2/medialib/Image_Bank/CH16/FG16_03.jpg

  19. History of Bone Marrow Transplants • Conceived in a dog kennel in Cooperstown, NY during the 1950s • RBCs could be successfully transfused from compatible donor to needy recipient • Marrow cells could not: Body identified them as foreign invaders and destroyed them • Hiroshima – one reason that radiation was so deadly because it destroyed the bone-marrow cells of its victims – hemorrhage, infection • Need: ability to restore bone marrow

  20. History of Bone Marrow Transplants • E. Donnal Thomas • Grew up in Texas, attended Harvard Med School • Treated leukemia patients with chemotherapy • Believed that providing new, healthy bone marrow cells was essential to curing leukemia • Tested various transplant techniques in dogs • Tested them in patients with late stage leukemia • Every patient who underwent transplantation died during the procedure of shortly thereafter. After 4 years stopped human trials. • “Things were pretty grim.”

  21. History of Bone Marrow Transplants • E. Donnal Thomas • 8 years later, identified genetic markers on WBCs of histocompatibility • Enabled close matching of donor and recipient • Led to successful results in dogs • Resumed human trials • Led to successful treatment for leukemia • Received the Nobel Prize in 1990 http://research.mednet.ucla.edu/images/nobel_med.gif

  22. Bone Marrow Transplants: Leukemia • Courtney Stevens • High school sophomore with leukemia • Treated with a bone marrow transplant “It was a complete nightmare. For days, I’d be on all fours and just retch and retch.” “I looked like a lobster, and thought I had bugs crawling on me. I’d hit myself and scream.” “ I was in that sterile bubble, and forgot what skin against skin felt like. That was lost. I just wanted to hold on to my mom or dad, like a two-year-old, and I couldn’t” “I had terrible diarrhea, a blistering rash all over my body, and jaundice. I was the color of an egg yolk.” http://www.jeromegroopman.com/articles/bone-marrow-transplant.html

  23. Bone Marrow Transplants: Breast CA • Chemotherapy is often ineffective for Stage IV breast cancer • Would higher doses of chemotherapy be more effective? • Requires bone marrow transplant • Can do autologous transplant (use patient’s own bone marrow) • HDCT + BMT: • Harvest stem cells from patient • Give HDCT • Perform autologus stem cell transplant (ASCT) • Expensive, high morbidity and mortality

  24. Bone Marrow Transplants: Breast CA • Tamar Lowenstein • 39 yo lawyer with widely metastatic breast cancer • Treated with HDCT and bone marrow transplant • Peripheral blood stem cell transplantation “It’s getting worse every hour.” Lips were so blistered that speaking was painful Chemical burn throughout her entire GI tract “I wish I hadn’t done it. It was a mistake.” Could not eat for 5 weeks. Weight dropped 46 lbs Tumor did respond to therapy http://www.jeromegroopman.com/articles/bone-marrow-transplant.html

  25. PBSC Transplantation with Apheresis • Where are stem cells? • Most stem cells are found in the bone marrow, • Some, called peripheral blood stem cells (PBSCs), can be found in blood • Apheresis: • Patient given medication to increase the # of stem cells released into the bloodstream • Blood is removed through a central venous catheter • Blood goes through machine that removes stem cells • Blood is returned to patient and collected cells stored

  26. “The Equipment” “The Centrifuge” http://www.rush.edu/bone-marrow/autologous/images/graft3.jpg

  27. Blood components are separated by centrifugal force. Packed Red Blood Cell Layer Plasma Layer Buffy Coat Layer Containing Progenitor Cells Stem Cell Collection Port

  28. Identification of Stem Cells • Stem cells cannot be distinguished from other cells in the bone marrow using a simple microscope.

  29. Flow Cytometry: • Stem cells express a certain protein on the surface of their cells: • CD34 • CD34+ cells are measured using a flow cytometer • Sophisticated test • Takes several hours

  30. Need 5 million stem cells/kg body weight. 0.1—1.0% of collected cells are peripheral blood stem cells. Over 20L of blood must be processed. The entire blood volume must be treated four times.

  31. Clinical Trials of HDCT + BMT • 1980-1990: • Phase II Trials with historical controls • Pts with metastatic breast cancer treated with HDC+BMT • 40% improvement in 3-yr survival compared to historical controls treated with standard chemo • Increased adverse effects: high mortality (0-22%) and morbidity • Increased cost: $160,000 (now $60,000) • Selection bias?? • Only included patients that responded to initial standard-dose chemotherapy • Prospects better for treating responsive disease

  32. Science vs. Politics • Media coverage • Patients demands • Legal cases • Legislation • Insurance coverage

  33. Timeline • 1991: 60 Minutes • Aired piece decrying Aetna’s decision to deny coverage for HDCT+BMT for breast CA • 1993: • Nelene Fox (38 yo mother of 3) sued HealthNet for failure to provide coverage for HDC+BMT • HealthNet paid for a relative of its CEO to receive HDC+BMT, but denied coverage to Fox and others • Fox’s family raised $210k for the transplant • Fox died of breast cancer before the verdict • Fox’s family was awarded $89M, largest jury verdict against an HMO at the time • Received wide publicity

  34. Timeline • 1993: • Massachusetts legislature mandated benefit law for HDC+BMT • 1994: • Insurers approve 77% of breast cancer patient requests for HDC+BMT clinical trial participation • Approval is highly arbitrary, even for similar patients covered by the same insurer • 9 of 12 large insurers surveyed say threat of litigation was a major factor in their decision to provide coverage

  35. Timeline • 1995: • Small (90 pts), short randomized trial by Bezwoda showed survival benefit for HDCT+BMT for metastatic breast cancer • More than 80% of American physicians believe that women with metastatic breast cancer should be treated with HDCT+BMT • 1990s: • More than 41,000 patients underwent HDCT+BMT for breast cancer despite a paucity of clinical evidence regarding effectiveness • Difficult to recruit patients to randomized Phase III clinical trials (took twice as long to complete as planned)

  36. Timeline • 1999: • American Society of Clinical Oncology Meeting • Results of 5 randomized clinical trials reported • Four studies showed no survival benefit with BMT; some showed it took longer for cancer to return • One South African study showed survival benefit • 83% five year survival for BMT • 65% five year survival for controls • 100 months average disease free survival for BMT • 47.5 months average disease free survival for controls • 1999 NY Times articles • Doubts Raised on a Breast Cancer Procedure By DENISE GRADY April 16, 1999, Friday • NPR Story • http://www.npr.org/templates/story/story.php?storyId=1049404

  37. Insurance Coverage • Anthem Insurance • 1996-1998: # requests for BMT increased from 64 to 83 per year • 1999: company expanded indications for which they would approve BMT • 1999: Results of RCTs released • 1999: Only 42 requests for BMT (only 4 requests in last 5 months of 1999) • Most insurance companies now cover HDCT+ BMT for breast cancer as part of FDA or NCI sponsored clinical trial • http://www.aetna.com/cpb/medical/data/500_599/0507.html

  38. RCT Results

  39. RCT Results

  40. RCT Results

  41. Why was only one study positive? • Team of scientists sent to audit trial results • Study showed little evidence of randomization • Records for many patients could not be found • Many patients did not meet eligibility criteria • Trial was not approved by the University’s IRB • No signed informed consents forms • University conducted formal ethics inquiry • Dr. Bezwoda admitted “serious breach of scientific honesty and integrity” • University fired Dr. Bezwoda

  42. Current Thinking • Appears to be no survival benefit to HDCT+BMT • 3 years • 5 years • There is a significant increase in disease free survival at 3 years with HDCT+ BMT • This increase disappears at 5 years • Side effects are more common with HDCT+BMT, most are reversible • Quality of life is lower at 6 months, but similar at 1 year

  43. Technology Assessment • Biological Plausibility • Does the biology support the technology? • Technical Feasibility • Safely and reliably deliver technology to patients? • Clinical Trials • Sensitivity & specificity in a relevant population? • Disease-free survival & 5-year survival in a relevant population? • Patient Outcomes • Does the technology improve the patient’s health? • Societal Outcomes • Cost and ethical implications of the technology? Littenberg B. Technology Assessment in Medicine. Academic Med 67:424, 1992

  44. Science of Understanding Disease Emerging Health Technologies Bioengineering Preclinical Testing Ethics of research Adoption & Diffusion Clinical Trials • Abandoned due to: • poor performance • safety concerns • ethical concerns • legal issues • social issues • economic issues Cost-Effectiveness

  45. What are the dangers of allowing political pressures to overwhelm science?What is the proper forum to resolve controversies?

  46. “In an era in which technological imperative is one of the most powerful drivers of health care costs, these are crucial lessons.”

  47. More Research? • Longer follow up may show advantages of high dose therapy • There may be sub-groups of women who benefit from high dose therapy • HER-2/neu negative tumors • 10 or more positive axillary nodes • Better technology to eliminate cancer cells from stem cell transplants

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